O1-conotoxin Tx6.7 cloned from the genomic DNA of Conus textile that inhibits calcium currents.

Maojun Zhou, Manyi Yang, Huiling Wen, Shun Xu, Cuifang Han, Yun Wu
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Abstract

Background: Conotoxins exhibit great potential as neuropharmacology tools and therapeutic candidates due to their high affinity and specificity for ion channels, neurotransmitter receptors or transporters. The traditional methods to discover new conotoxins are peptide purification from the crude venom or gene amplification from the venom duct.

Methods: In this study, a novel O1 superfamily conotoxin Tx6.7 was directly cloned from the genomic DNA of Conus textile using primers corresponding to the conserved intronic sequence and 3' UTR elements. The mature peptide of Tx6.7 (DCHERWDWCPASLLGVIYCCEGLICFIAFCI) was synthesized by solid-phase chemical synthesis and confirmed by mass spectrometry.

Results: Patch clamp experiments on rat DRG neurons showed that Tx6.7 inhibited peak calcium currents by 59.29 ± 2.34% and peak potassium currents by 22.33 ± 7.81%. In addition, patch clamp on the ion channel subtypes showed that 10 μM Tx6.7 inhibited 56.61 ± 3.20% of the hCaV1.2 currents, 24.67 ± 0.91% of the hCaV2.2 currents and 7.30 ± 3.38% of the hNaV1.8 currents. Tx6.7 had no significant toxicity to ND7/23 cells and increased the pain threshold from 0.5 to 4 hours in the mouse hot plate assay.

Conclusion: Our results suggested that direct cloning of conotoxin sequences from the genomic DNA of cone snails would be an alternative approach to obtaining novel conotoxins. Tx6.7 could be used as a probe tool for ion channel research or a therapeutic candidate for novel drug development.

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从松果纤维基因组DNA中克隆出抑制钙电流的O1-conotoxin Tx6.7。
背景:由于其对离子通道、神经递质受体或转运体的高亲和力和特异性,Conotoxins作为神经药理学工具和治疗候选者具有很大的潜力。发现新的concontoxin的传统方法是从粗毒液中提纯多肽或从蛇毒管中扩增基因。方法:利用保守内含子序列和3′UTR序列对应的引物,直接从Conus纺织品基因组DNA中克隆出一种新的O1超家族concontoxin Tx6.7。采用固相化学合成方法合成Tx6.7成熟肽(DCHERWDWCPASLLGVIYCCEGLICFIAFCI),并采用质谱法对其进行确证。结果:膜片钳实验显示,Tx6.7对大鼠DRG神经元钙电流峰值和钾电流峰值的抑制作用分别为59.29±2.34%和22.33±7.81%。此外,对离子通道亚型进行膜片钳实验表明,10 μM Tx6.7对hCaV1.2、hCaV2.2和hNaV1.8电流的抑制分别为56.61±3.20%、24.67±0.91%和7.30±3.38%。在小鼠热板实验中,Tx6.7对ND7/23细胞无明显毒性作用,并使小鼠疼痛阈值从0.5小时增加到4小时。结论:从锥螺基因组DNA中直接克隆螺毒素序列是获得新型螺毒素的另一种途径。Tx6.7可作为离子通道研究的探针工具或新药开发的治疗候选物。
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来源期刊
CiteScore
4.80
自引率
8.30%
发文量
39
审稿时长
6-12 weeks
期刊介绍: Journal of Venomous Animals and Toxins including Tropical Diseases (JVATiTD) is a non-commercial academic open access publication dedicated to research on all aspects of toxinology, venomous animals and tropical diseases. Its interdisciplinary content includes original scientific articles covering research on toxins derived from animals, plants and microorganisms. Topics of interest include, but are not limited to:systematics and morphology of venomous animals;physiology, biochemistry, pharmacology and immunology of toxins;epidemiology, clinical aspects and treatment of envenoming by different animals, plants and microorganisms;development and evaluation of antivenoms and toxin-derivative products;epidemiology, clinical aspects and treatment of tropical diseases (caused by virus, bacteria, algae, fungi and parasites) including the neglected tropical diseases (NTDs) defined by the World Health Organization.
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